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An otoprotective role for the apoptosis inhibitor protein survivin
Authors:S K Knauer  U-R Heinrich  C Bier  N Habtemichael  D Docter  K Helling  W J Mann  and R H Stauber
Institution:1Department of Molecular and Cellular Oncology, University Hospital of Mainz, Langenbeckstrasse 1, Mainz 55101, Germany;2Department for Molecular Biology II, Centre for Medical Biotechnology (ZMB), University Duisburg-Essen, Universitätsstraße, Essen 45117, Germany;3Department of Otorhinolaryngology, Head and Neck Surgery, University Hospital of Mainz, Langenbeckstrasse 1, Mainz 55101, Germany
Abstract:Hearing impairment caused by ototoxic insults, such as noise or gentamicin is a worldwide health problem. As the molecular circuitries involved are not yet resolved, current otoprotective therapies are rather empirical than rational. Here, immunohistochemistry and western blotting showed that the cytoprotective protein survivin is expressed in the human and guinea pig cochlea. In the guinea pig model, moderate noise exposure causing only a temporary hearing impairment transiently evoked survivin expression in the spiral ligament, nerve fibers and the organ of Corti. Mechanistically, survivin upregulation may involve nitric oxide (NO)-induced Akt signaling, as enhanced expression of the endothelial NO synthase and phosphorylated Akt were detectable in some surviving-positive cell types. In contrast, intratympanic gentamicin injection inducing cell damage and permanent hearing loss correlated with attenuated survivin levels in the cochlea. Subsequently, the protective activity of the human and the guinea pig survivin orthologs against the ototoxin gentamicin was demonstrated by ectopic overexpression and RNAi-mediated depletion studies in auditory cells in vitro. These data suggest that survivin represents an innate cytoprotective resistor against stress conditions in the auditory system. The pharmacogenetic modulation of survivin may thus provide the conceptual basis for the rational design of novel therapeutic otoprotective strategies.
Keywords:Auditory system  aminoglycoside antibiotics  chromosomal passenger complex  cochlea  nitric oxide  ototoxicity
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